4.2 Article

A polysaccharide from Grifola frondosa relieves insulin resistance of HepG2 cell by Akt-GSK-3 pathway

Journal

GLYCOCONJUGATE JOURNAL
Volume 31, Issue 5, Pages 355-363

Publisher

SPRINGER
DOI: 10.1007/s10719-014-9526-x

Keywords

Grifola frondosa polysaccharide; Hypoglycemic activity; Insulin resistance; Akt/p-Akt; GSK-3

Funding

  1. [2012BAD33B04]
  2. [2012AA022108]
  3. [2012GB2A100016]
  4. [IRT1166]
  5. [31000768]
  6. [31171731]
  7. [10ZCZDSY07000]

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Grifola frondosa is an important fungal research resource. However, there was little report about hyperglycemic activity of Grifola frondosa polysaccharide on insulin resistance in vitro. In this study, the hypoglycemic activity of a polysaccharide obtained from Grifola frondosa (GFP) on HepG2 cell and hpyerglycemic mechanism were investigated. The purity of the isolated polysaccharides was examined by HPLC. In this research, it was found that GFP enhanced the absorption of glucose of HepG2 cells in a dose dependent manner at 24 h of 30 ugmL(-1). GC-MS and FT-IR spectroscopy analysis results showed that glucose and galactose were the dominant monosaccharides in GFP and the major component of GFP was beta-pyranoside. Western-blotting results showed that the HepG2 cell model treated with GFP activated the insulin receptor protein (IRS) in the cell membrane and increased phosphorylated-AktSer473 expression, which had an inhibition of glycogen synthase kinase (GSK-3). The down-regulation of GSK-3 stimulated synthesis of intracellular glycogen. The results above suggested that the GFP increased the metabolism of glucose and stimulated synthesis of intracellular glycogen through the Akt/GSK-3 pathway.

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